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Use of a cocktail of monoclonal antibodies and human complement in selective killing of acute lymphocytic leukemia cells

✍ Scribed by Kenichi Sugita; Otto Majdic; Hannes Stockinger; Wolfgang Holter; Ursula Köller; Christian Peschel; Walter Knapp


Publisher
John Wiley and Sons
Year
1986
Tongue
French
Weight
691 KB
Volume
37
Category
Article
ISSN
0020-7136

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✦ Synopsis


Autologous remission bone marrow is a potential source of repopulative stem cells after ablative chemoradiotherapy of tumor patients. Even with remission bone marrow, one major obstacle to use of autologous bone-marrow support is the danger of reinfusing viable tumor cells. This report describes a purging protocol with human complement, which seems suitable for eliminating acute lymphatic leukemia (ALL) cells of the common ALL type. Lysis of ALL blasts is induced with a cocktail of 3 monoclonal antibodies of IgM type (termed VIB-pool). These are directed against the CALLA (CDIO) antigen (VIL-AI antibody) and against 2 different epitopes of the CD24 surface structure (VlLC5 and VIB-E3 antibodies). The purging efficiency was evaluated with leukemic cell lines of the common ALL type (Reh-6 and Nalm-6) and with blast cells from common ALL patients. Optimal lysis was obtained with antibody and human serum concentrations as low as I pglml and 7% respectively. As a standard purging protocol we propose one 20min incubation at room temperature with antibody followed by two 30-min incubations at 37OC with 25% human complement. In dye exclusion tests 99% purging efficiency and in clonogenic assays detecting elimination of up to 5 logs of clonogenic tumor cells 99.99% (= 4 logs) purging efficiency were achieved. Treatment with VIB-pool and human complement had no negative effect on the growth of the normal hemopoietic progenitor cells CFU-GM, CFU-E and BFU-E.


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